Table 17d. Antiretroviral Therapy-Associated Adverse Effects and Management Recommendations—Hematologic Effects

Onset

• Variable; weeks to months after starting therapy

Presentation

More Common

• Asymptomatic
• Mild fatigue
• Pallor
• Tachypnea

Rare

• Congestive heart failure

Newborns Exposed to HIV

• Severe anemia is uncommon but might be coincident with physiologic Hgb nadir.

Children with HIV Who Are Taking ARV Drugs

• Anemia is two to three times more common with ZDV-containing regimens than with all other regimens.

Newborns Exposed to HIV

• Premature birth is the most common risk factor.
• In utero exposure to ZDV-containing regimens
• Advanced maternal HIV
• Neonatal blood loss
• Combination ARV prophylaxis or presumptive HIV therapy, although no particular regimen has been identified as being worse than others.

Children with HIV Who Are Taking ARV Drugs

• Underlying hemoglobinopathy (e.g., sickle cell disease, G6PD deficiency)
• Myelosuppressive drugs (e.g., TMP-SMX, rifabutin)
• Iron deficiency
• Advanced or poorly controlled HIV disease
• OIs of the bone marrow
• Malnutrition

Newborns Exposed to HIV

• Obtain CBC at birth.
• Consider repeating CBC at 4 weeks for neonates who are at higher risk (e.g., those born prematurely or who are known to have low birth Hgb) and for neonates who receive ZDV beyond 4 weeks.

Children with HIV Who Are Taking ARV Drugs

• Avoid using ZDV in children with severe anemia when alternative agents are available.
• Obtain CBC as part of routine care (see Clinical and Laboratory Monitoring of Pediatric HIV Infection).

Newborns Exposed to HIV

• Anemia rarely requires intervention unless it is symptomatic or Hgb <7.0 g/dL.
• ZDV administration can be limited to 4 weeks in low-risk neonates (see Antiretroviral Management of Newborns with Perinatal HIV Exposure or HIV Infection).

Children with HIV Who Are Taking ARV Drugs

• Discontinue non-ARV, marrow-toxic drugs, if feasible.
• Treat coexisting iron deficiency, OIs, and malignancies.
• For persistent, severe anemia that is thought to be associated with ARV drugs (typically macrocytic anemia), switch to a regimen that does not contain ZDV.

Onset

• Within days or weeks of starting therapy

Presentation

• Asymptomatic, but MCV often is >100 fL
• Sometimes associated with or may progress to anemia

Onset

• Variable

Presentation

• Asymptomatic

Newborns Exposed to HIV

• Rare

Children with HIV Who Are Taking ARV Drugs

• 2% to 4% of children on ARV drugs
• Highest rates occur in children on ZDV-containing regimens

Newborns Exposed to HIV

• In utero exposure to ARV drugs
• Combination ARV prophylaxis, particularly ZDV plus 3TC and NVP

Children with HIV Who Are Taking ARV Drugs

• Advanced or poorly controlled HIV infection
• Myelosuppressive drugs (e.g., TMP-SMX, ganciclovir, hydroxyurea, rifabutin)

Children with HIV Who Are Taking ARV Drugs

• Obtain CBC as part of routine care.

Newborns Exposed to HIV

• No established threshold for intervention; some experts would consider using an alternative NRTI for prophylaxis if ANC reaches <500 cells/mm³. ZDV administration can be limited to 4 weeks in low-risk neonates (see Antiretroviral Management of Newborns with Perinatal HIV Exposure or HIV Infection).

Children with HIV Who Are Taking ARV Drugs

• Discontinue non-ARV, marrow-toxic drugs, if feasible.
• Treat coexisting OIs and malignancies.
• In cases of persistent, severe neutropenia that is thought to be associated with ARV drugs, switch to a regimen that does not contain ZDV.